Distinct inactive conformations of the dopamine D2 and D3 receptors correspond to different extents of inverse agonism

Lane, J. Robert; Abramyan, Ara M.; Adhikari, Pramisha; Keen, Alastair C.; Lee, Kuo-Hao; Verma, Ravi Kumar; Lim, Herman D.; Yano, Hideaki; Javitch, Jonathan A.; Shi, Lei

doi:10.7554/elife.52189

Cited by 33 publications

(48 citation statements)

References 56 publications

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“…2,[21][22][23] Likewise, mutation of Trp100 ECL1 Ala increases the association and dissociation of antagonist ligand risperidone. 24 The hD3 simulations lead to a very similar result (Fig. S2b, ESI †).…”

supporting

confidence: 54%

Controlling receptor function from the extracellular vestibule of G-protein coupled receptors

et al. 2020

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supporting

confidence: 54%

Controlling receptor function from the extracellular vestibule of G-protein coupled receptors

et al. 2020

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“…Indeed, ECL2 in 5-HT 2A R moves slightly to bind a different ligand 26 . An MD simulation study also suggested these dynamics of the ECL2 of D 2 R 47 and reported that the helical conformation of ECL2 observed in D 2 R ris tended to unwind toward an extended conformation, similar to that of D 3 R eti , regardless of the bound ligand, including spiperone, risperidone, or eticlopride 47 . The unwinding involves a drastic rearrangement of the side chain of Ile183 45.51 , dissociating from a hydrophobic pocket.…”

Section: Discussionmentioning

confidence: 87%

Structure of the dopamine D2 receptor in complex with the antipsychotic drug spiperone

Inoue

Fujiwara

et al. 2020

Nat Commun

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In addition to the serotonin 5-HT2A receptor (5-HT2AR), the dopamine D2 receptor (D2R) is a key therapeutic target of antipsychotics for the treatment of schizophrenia. The inactive state structures of D2R have been described in complex with the inverse agonists risperidone (D2Rris) and haloperidol (D2Rhal). Here we describe the structure of human D2R in complex with spiperone (D2Rspi). In D2Rspi, the conformation of the extracellular loop (ECL) 2, which composes the ligand-binding pocket, was substantially different from those in D2Rris and D2Rhal, demonstrating that ECL2 in D2R is highly dynamic. Moreover, D2Rspi exhibited an extended binding pocket to accommodate spiperone’s phenyl ring, which probably contributes to the selectivity of spiperone to D2R and 5-HT2AR. Together with D2Rris and D2Rhal, the structural information of D2Rspi should be of value for designing novel antipsychotics with improved safety and efficacy.

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“…Thus no main difference was expected. In reality the results show differences in D2 inactive conformation that suggest different receptor inactive states ( Lane et al., 2020 ). In addition the agonist binding pocket in the D2 allows an extension that has been used to study D2 > D3 and D4 selectivity (with agonist ligands) and to determine the possibility to obtain biased agonists for D2 ( Fan et al., 2020 ).…”

Section: Section 3 Dr Ligands and Scz Therapies The New Wave Of Ligmentioning

confidence: 99%

Dopamine Receptor Subtypes, Physiology and Pharmacology: New Ligands and Concepts in Schizophrenia

Martel¹,

McArthur²

2020

Front. Pharmacol.

150

125

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Dopamine receptors are widely distributed within the brain where they play critical modulator roles on motor functions, motivation and drive, as well as cognition. The identification of five genes coding for different dopamine receptor subtypes, pharmacologically grouped as D1- (D1 and D5) or D2-like (D2S, D2L, D3, and D4) has allowed the demonstration of differential receptor function in specific neurocircuits. Recent observation on dopamine receptor signaling point at dopamine—glutamate-NMDA neurobiology as the most relevant in schizophrenia and for the development of new therapies. Progress in the chemistry of D1- and D2-like receptor ligands (agonists, antagonists, and partial agonists) has provided more selective compounds possibly able to target the dopamine receptors homo and heterodimers and address different schizophrenia symptoms. Moreover, an extensive evaluation of the functional effect of these agents on dopamine receptor coupling and intracellular signaling highlights important differences that could also result in highly differentiated clinical pharmacology. The review summarizes the recent advances in the field, addressing the relevance of emerging new targets in schizophrenia in particular in relation to the dopamine – glutamate NMDA systems interactions.

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Distinct inactive conformations of the dopamine D2 and D3 receptors correspond to different extents of inverse agonism

Cited by 33 publications

References 56 publications

Controlling receptor function from the extracellular vestibule of G-protein coupled receptors

Controlling receptor function from the extracellular vestibule of G-protein coupled receptors

Structure of the dopamine D2 receptor in complex with the antipsychotic drug spiperone

Dopamine Receptor Subtypes, Physiology and Pharmacology: New Ligands and Concepts in Schizophrenia

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